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胆固醇和胆甾烷醇晶体上羟基磷灰石(Ca-HAp)在模拟体液中的生长:对动脉粥样硬化相关病理性钙化的一种可能见解。

Growth of calcium hydroxyapatite (Ca-HAp) on cholesterol and cholestanol crystals from a simulated body fluid: A possible insight into the pathological calcifications associated with atherosclerosis.

作者信息

Laird Dougal F, Mucalo Michael R, Yokogawa Yoshiyuki

机构信息

Chemistry Department, University of Waikato, Private Bag 3105, Hamilton 2020, New Zealand.

出版信息

J Colloid Interface Sci. 2006 Mar 15;295(2):348-63. doi: 10.1016/j.jcis.2005.09.013. Epub 2005 Oct 17.

Abstract

An experimental study into calcium phosphate (CP) nucleation and growth on cholesterol and cholestanol surfaces from a supersaturated simulated body fluid (SBF) is presented with the overall aim of gaining some fundamental insights into the pathological calcifications associated with atherosclerosis. Soaking of pressed cholesterol disks at physiological temperature in SBF solutions was found to lead to CP nucleation and growth if the disks were surface roughened and if an SBF with concentrations of the calcium and hydrogen phosphate ions at 2.25x physiological concentrations was used. The CP phase deposited was shown via SEM micrographs to possess a florette type morphology akin to that observed in earlier reported studies. The use of recrystallised cholesterol and cholestanol microcrystals as substrates for soaking in SBF facilitated the observation of CP deposition. In general, cholesterol recrystallised from polar solvents like 95% ethanol as a cholesterol monohydrate phase which was a better substrate for CP growth than cholesterol recrystallised from more non-polar solvents (e.g., benzene) which produced anhydrous cholesterol phases. CP was also observed to form on recrystallised cholestanol microcrystals, a molecule closely related to cholesterol. Inductively coupled plasma optical emission spectrometry (ICP-OES) data gave confirmation that Ca:P mole ratios of the grown CP were 1.3-1.5 suggesting a mixed phase of octacalcium phosphate (OCP) and Ca-deficient HAp and that the CP coating grows (with time of soaking) on the substrates after nucleation in the SBF growth medium. Infrared (IR) spectra of the extracted coatings from the cholesterol substrates confirmed that the CP phase deposited is a semi crystalline HAp with either carbonate substituted into its structure or else co-deposited as calcium carbonate. Soaking experiments involving modified cholesterol substrates in which the OH group in the molecule was replaced with the oleiyl or phosphonate group showed no CP nucleation and growth. This observation illustrates the importance of the known epitaxial relationship between cholesterol and HAp (which theoretically predicts favourable deposition of one phase upon the other) and the consequences of its destruction (by chemical modification of the cholesterol). In the case of the phosphorylated cholesterol, failure of this substrate to nucleate CP phases may have also been caused by the reduction in concentration of free solution Ca2+ in the SBF medium by complexation with the phosphonate groups on the phosphorylated cholesterol. This would have reduced the ion product of Ca2+ and inorganic phosphate and lowered the degree of supersaturation in the SBF medium.

摘要

本文介绍了一项关于磷酸钙(CP)在胆固醇和胆甾烷醇表面从过饱和模拟体液(SBF)中形核和生长的实验研究,其总体目标是深入了解与动脉粥样硬化相关的病理性钙化的一些基本情况。研究发现,如果将压制的胆固醇圆盘在生理温度下浸泡在SBF溶液中,且圆盘表面粗糙,并使用钙和磷酸氢根离子浓度为生理浓度2.25倍的SBF,则会导致CP形核和生长。通过扫描电子显微镜(SEM)照片显示,沉积的CP相具有小花状形态,类似于早期报道研究中观察到的形态。使用重结晶的胆固醇和胆甾烷醇微晶作为浸泡在SBF中的底物,便于观察CP沉积。一般来说,从极性溶剂如95%乙醇中重结晶的胆固醇为一水合胆固醇相,它比从更多非极性溶剂(如苯)中重结晶的无水胆固醇相更有利于CP生长。在与胆固醇密切相关的分子重结晶胆甾烷醇微晶上也观察到CP形成。电感耦合等离子体发射光谱(ICP - OES)数据证实,生长的CP的钙磷摩尔比为1.3 - 1.5,表明是磷酸八钙(OCP)和缺钙羟基磷灰石(HAp)的混合相,且CP涂层在SBF生长介质中形核后在底物上(随着浸泡时间)生长。从胆固醇底物中提取的涂层的红外(IR)光谱证实,沉积的CP相是一种半结晶的HAp,其结构中要么有碳酸盐取代,要么与碳酸钙共沉积。涉及将分子中的OH基团替换为油基或膦酸酯基团的改性胆固醇底物的浸泡实验表明没有CP形核和生长。这一观察结果说明了胆固醇与HAp之间已知的外延关系(理论上预测一相在另一相上的有利沉积)的重要性以及其破坏(通过胆固醇的化学改性)的后果。对于磷酸化胆固醇,该底物未能使CP相成核也可能是由于SBF介质中游离溶液Ca2 +浓度因与磷酸化胆固醇上的膦酸酯基团络合而降低所致。这会降低Ca2 +与无机磷酸盐的离子积,并降低SBF介质中的过饱和度。

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